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疾病的昆虫传播媒介:新抗菌药物的未开发宝库?

Insect Vectors of Disease: Untapped Reservoirs for New Antimicrobials?

作者信息

Tobias Nicholas J

机构信息

Molekulare Biotechnologie, Fachbereich Biowissenschaften, Goethe-Universität Frankfurt Frankfurt am Main, Germany.

出版信息

Front Microbiol. 2016 Dec 22;7:2085. doi: 10.3389/fmicb.2016.02085. eCollection 2016.

DOI:10.3389/fmicb.2016.02085
PMID:28066398
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5177651/
Abstract

With the increase in antibiotic resistance among infectious diseases, the need for new strategies for identifying compounds with inhibitory effects is dire. Traditional methods of genome sequencing and systematic characterization of potential antimicrobial gene clusters, although effective, are unfortunately not yielding results at a speed consistent with the rise in antimicrobial resistance. One approach could be to use a more targeted approach to antimicrobial compound discovery. Insect vectors often mediate the transmissions of parasitic infections for example, leishmaniasis, malaria, and trypanosomiasis. Within the insect, among the pathogens, are commensal and/or obligate symbiotic bacteria, which often undergo a population shift upon colonization of the insect host. The remaining bacteria may be either resistant to the effects of the respective parasites, or possibly essential for a successful colonization and continued spread of the parasite due to an obligate symbiosis between bacteria and insect host. Interestingly, these shifts are often toward groups of bacteria known to harbor many polyketide synthase and non-ribosomal peptide synthetase gene clusters involved in bioactive molecule production. This perspective explores the possibility to exploit the natural interactions between parasite, symbiont, and insect host for a more targeted approach toward natural product discovery, in an environment where potential compound producers are naturally interfacing with human pathogens.

摘要

随着传染病中抗生素耐药性的增加,迫切需要新的策略来鉴定具有抑制作用的化合物。传统的基因组测序方法以及对潜在抗菌基因簇的系统表征方法虽然有效,但遗憾的是,其产生结果的速度与抗菌耐药性的上升不一致。一种方法可能是采用更具针对性的方法来发现抗菌化合物。例如,昆虫媒介常常介导利什曼病、疟疾和锥虫病等寄生虫感染的传播。在昆虫体内,在病原体之中,存在着共生和/或专性共生细菌,这些细菌在昆虫宿主定殖后常常会发生种群变化。剩余的细菌可能对相应寄生虫的影响具有抗性,或者由于细菌与昆虫宿主之间的专性共生关系,可能对寄生虫的成功定殖和持续传播至关重要。有趣的是,这些变化往往朝着已知含有许多参与生物活性分子生产的聚酮合酶和非核糖体肽合成酶基因簇的细菌群体发展。在潜在化合物生产者与人类病原体自然相互作用的环境中,本观点探讨了利用寄生虫、共生体和昆虫宿主之间的自然相互作用,以采用更具针对性的方法来发现天然产物的可能性。

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